A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure
Gulf War Illness (GWI) is a chronic multisymptom illness with a central nervous system component that includes memory impairment as well as neurological and musculoskeletal deficits. Previous studies have shown that in the First Persian Gulf War conflict (1990-1991) exposure to Gulf War (GW) agents,...
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doaj-a27ce4356f684b0992a56bd554bdd7c22020-11-25T00:37:39ZengFrontiers Media S.A.Frontiers in Integrative Neuroscience1662-51452016-01-01910.3389/fnint.2015.00071159632A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposureZuchra eZakirova0Zuchra eZakirova1Zuchra eZakirova2Gogce eCrynen3Gogce eCrynen4Samira eHassan5Laila eAbdullah6Laila eAbdullah7Laila eAbdullah8Lauren eHorne9Venkatarajan eMathura10Venkatarajan eMathura11Fiona eCrawford12Fiona eCrawford13Fiona eCrawford14Ghania eAit-Ghezala15Ghania eAit-Ghezala16Ghania eAit-Ghezala17The Roskamp InstituteThe Open UniversityJames A. Haley Veterans HospitalThe Roskamp InstituteThe Open UniversityThe Roskamp InstituteThe Roskamp InstituteThe Open UniversityJames A. Haley Veterans HospitalThe Roskamp InstituteThe Roskamp InstituteThe Open UniversityThe Roskamp InstituteThe Open UniversityJames A. Haley Veterans HospitalThe Roskamp InstituteThe Open UniversityJames A. Haley Veterans HospitalGulf War Illness (GWI) is a chronic multisymptom illness with a central nervous system component that includes memory impairment as well as neurological and musculoskeletal deficits. Previous studies have shown that in the First Persian Gulf War conflict (1990-1991) exposure to Gulf War (GW) agents, such as pyridostigmine bromide (PB) and permethrin (PER), were key contributors to the etiology of GWI.For this study, we used our previously established mouse model of GW agent exposure (10 days PB+PER) and undertook an extensive lifelong neurobehavioral characterization of the mice from 11 days to 22.5 months post exposure in order to address the persistence and chronicity of effects suffered by the current GWI patient population, 24 years post-exposure. Mice were evaluated using a battery of neurobehavioral testing paradigms, including Open Field Test, Elevated Plus Maze, Three Chamber Testing, Radial Arm Water Maze and Barnes Maze Test. We also carried out neuropathological analyses at 22.5 months post exposure to GW agents after the final behavioral testing. Our results demonstrate that PB+PER exposed mice exhibit neurobehavioral deficits beginning at the 13 months post exposure time point and continuing trends through the 22.5 month post exposure time point. Furthermore, neuropathological changes, including an increase in GFAP staining in the cerebral cortices of exposed mice, were noted 22.5 months post exposure. Thus, the persistent neuroinflammation evident in our model presents a platform with which to identify novel biological pathways, correlating with emergent outcomes that may be amenable to therapeutic targeting. Furthermore, in this work we confirmed our previous findings that GW agent exposure causes neuropathological changes, and have presented novel data which demonstrate increased disinhibition, and lack of social preference in PB+PER exposed mice at 13 months after exposure. We also extended upon our previous work to cover the lifespan of the laboratory mouse using a battery of neurobehavioral techniques.http://journal.frontiersin.org/Journal/10.3389/fnint.2015.00071/fullmouse modelNeuropathologyGulf WarneurobehaviorPyridostigmine bromide (PB)Permethrin (PER) |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Zuchra eZakirova Zuchra eZakirova Zuchra eZakirova Gogce eCrynen Gogce eCrynen Samira eHassan Laila eAbdullah Laila eAbdullah Laila eAbdullah Lauren eHorne Venkatarajan eMathura Venkatarajan eMathura Fiona eCrawford Fiona eCrawford Fiona eCrawford Ghania eAit-Ghezala Ghania eAit-Ghezala Ghania eAit-Ghezala |
spellingShingle |
Zuchra eZakirova Zuchra eZakirova Zuchra eZakirova Gogce eCrynen Gogce eCrynen Samira eHassan Laila eAbdullah Laila eAbdullah Laila eAbdullah Lauren eHorne Venkatarajan eMathura Venkatarajan eMathura Fiona eCrawford Fiona eCrawford Fiona eCrawford Ghania eAit-Ghezala Ghania eAit-Ghezala Ghania eAit-Ghezala A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure Frontiers in Integrative Neuroscience mouse model Neuropathology Gulf War neurobehavior Pyridostigmine bromide (PB) Permethrin (PER) |
author_facet |
Zuchra eZakirova Zuchra eZakirova Zuchra eZakirova Gogce eCrynen Gogce eCrynen Samira eHassan Laila eAbdullah Laila eAbdullah Laila eAbdullah Lauren eHorne Venkatarajan eMathura Venkatarajan eMathura Fiona eCrawford Fiona eCrawford Fiona eCrawford Ghania eAit-Ghezala Ghania eAit-Ghezala Ghania eAit-Ghezala |
author_sort |
Zuchra eZakirova |
title |
A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure |
title_short |
A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure |
title_full |
A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure |
title_fullStr |
A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure |
title_full_unstemmed |
A chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of Gulf War agent exposure |
title_sort |
chronic longitudinal characterization of neurobehavioral and neuropathological cognitive impairment in a mouse model of gulf war agent exposure |
publisher |
Frontiers Media S.A. |
series |
Frontiers in Integrative Neuroscience |
issn |
1662-5145 |
publishDate |
2016-01-01 |
description |
Gulf War Illness (GWI) is a chronic multisymptom illness with a central nervous system component that includes memory impairment as well as neurological and musculoskeletal deficits. Previous studies have shown that in the First Persian Gulf War conflict (1990-1991) exposure to Gulf War (GW) agents, such as pyridostigmine bromide (PB) and permethrin (PER), were key contributors to the etiology of GWI.For this study, we used our previously established mouse model of GW agent exposure (10 days PB+PER) and undertook an extensive lifelong neurobehavioral characterization of the mice from 11 days to 22.5 months post exposure in order to address the persistence and chronicity of effects suffered by the current GWI patient population, 24 years post-exposure. Mice were evaluated using a battery of neurobehavioral testing paradigms, including Open Field Test, Elevated Plus Maze, Three Chamber Testing, Radial Arm Water Maze and Barnes Maze Test. We also carried out neuropathological analyses at 22.5 months post exposure to GW agents after the final behavioral testing. Our results demonstrate that PB+PER exposed mice exhibit neurobehavioral deficits beginning at the 13 months post exposure time point and continuing trends through the 22.5 month post exposure time point. Furthermore, neuropathological changes, including an increase in GFAP staining in the cerebral cortices of exposed mice, were noted 22.5 months post exposure. Thus, the persistent neuroinflammation evident in our model presents a platform with which to identify novel biological pathways, correlating with emergent outcomes that may be amenable to therapeutic targeting. Furthermore, in this work we confirmed our previous findings that GW agent exposure causes neuropathological changes, and have presented novel data which demonstrate increased disinhibition, and lack of social preference in PB+PER exposed mice at 13 months after exposure. We also extended upon our previous work to cover the lifespan of the laboratory mouse using a battery of neurobehavioral techniques. |
topic |
mouse model Neuropathology Gulf War neurobehavior Pyridostigmine bromide (PB) Permethrin (PER) |
url |
http://journal.frontiersin.org/Journal/10.3389/fnint.2015.00071/full |
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